DPAGT1 deficiency with encephalopathy (DPAGT1-CDG): Clinical and genetic description of 11 new patients

Bobby G. Ng; Hunter R. Underhill; Lars Palm; Per Bengtson; Jean Michel Rozet; Sylvie Gerber; Arnold Munnich; Xavier Zanlonghi; Cathy A. Stevens; Martin Kircher; Deborah A. Nickerson; Kati J. Buckingham; Kevin D. Josephson; Jay Shendure; Michael J. Bamshad; Hudson H. Freeze; Erik A. Eklund

doi:10.1007/8904_2018_128

DPAGT1 deficiency with encephalopathy (DPAGT1-CDG): Clinical and genetic description of 11 new patients

Bobby G. Ng, Hunter R. Underhill, Lars Palm, Per Bengtson, Jean Michel Rozet, Sylvie Gerber, Arnold Munnich, Xavier Zanlonghi, Cathy A. Stevens, Martin Kircher, Deborah A. Nickerson, Kati J. Buckingham, Kevin D. Josephson, Jay Shendure, Michael J. Bamshad, Hudson H. Freeze, Erik A. Eklund^*

^*Corresponding author for this work

Institute of Human Genetics

Abstract

Pathogenic mutations in DPAGT1 cause a rare type of a congenital disorder of glycosylation termed DPAGT1-CDG or, alternatively, a milder version with only myasthenia known as DPAGT1-CMS. Fourteen disease-causing mutations in 28 patients from 10 families have previously been reported to cause the systemic form, DPAGT1-CDG. We here report on another 11 patients from 8 families and add 10 new mutations. Most patients have a very severe disease course, where common findings are pronounced muscular hypotonia, intractable epilepsy, global developmental delay/intellectual disability, and early death. We also present data on three affected females that are young adults and have a somewhat milder, stable disease. Our findings expand both the molecular and clinical knowledge of previously published data but also widen the phenotypic spectrum of DPAGT1-CDG.

Original language	English
Title of host publication	JIMD Reports
Number of pages	8
Publisher	Springer
Publication date	2019
Pages	85-92
DOIs	https://doi.org/10.1007/8904_2018_128
Publication status	Published - 2019

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Ng, B. G., Underhill, H. R., Palm, L., Bengtson, P., Rozet, J. M., Gerber, S., Munnich, A., Zanlonghi, X., Stevens, C. A., Kircher, M., Nickerson, D. A., Buckingham, K. J., Josephson, K. D., Shendure, J., Bamshad, M. J., Freeze, H. H., & Eklund, E. A. (2019). DPAGT1 deficiency with encephalopathy (DPAGT1-CDG): Clinical and genetic description of 11 new patients. In JIMD Reports (pp. 85-92). (JIMD Reports; Vol. 44). Springer. https://doi.org/10.1007/8904_2018_128

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title = "DPAGT1 deficiency with encephalopathy (DPAGT1-CDG): Clinical and genetic description of 11 new patients",

abstract = "Pathogenic mutations in DPAGT1 cause a rare type of a congenital disorder of glycosylation termed DPAGT1-CDG or, alternatively, a milder version with only myasthenia known as DPAGT1-CMS. Fourteen disease-causing mutations in 28 patients from 10 families have previously been reported to cause the systemic form, DPAGT1-CDG. We here report on another 11 patients from 8 families and add 10 new mutations. Most patients have a very severe disease course, where common findings are pronounced muscular hypotonia, intractable epilepsy, global developmental delay/intellectual disability, and early death. We also present data on three affected females that are young adults and have a somewhat milder, stable disease. Our findings expand both the molecular and clinical knowledge of previously published data but also widen the phenotypic spectrum of DPAGT1-CDG.",

author = "Ng, {Bobby G.} and Underhill, {Hunter R.} and Lars Palm and Per Bengtson and Rozet, {Jean Michel} and Sylvie Gerber and Arnold Munnich and Xavier Zanlonghi and Stevens, {Cathy A.} and Martin Kircher and Nickerson, {Deborah A.} and Buckingham, {Kati J.} and Josephson, {Kevin D.} and Jay Shendure and Bamshad, {Michael J.} and Freeze, {Hudson H.} and Eklund, {Erik A.}",

note = "Publisher Copyright: {\textcopyright} Society for the Study of Inborn Errors of Metabolism (SSIEM) 2018.",

year = "2019",

doi = "10.1007/8904_2018_128",

language = "English",

series = "JIMD Reports",

publisher = "Springer",

pages = "85--92",

booktitle = "JIMD Reports",

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Ng, BG, Underhill, HR, Palm, L, Bengtson, P, Rozet, JM, Gerber, S, Munnich, A, Zanlonghi, X, Stevens, CA, Kircher, M, Nickerson, DA, Buckingham, KJ, Josephson, KD, Shendure, J, Bamshad, MJ, Freeze, HH & Eklund, EA 2019, DPAGT1 deficiency with encephalopathy (DPAGT1-CDG): Clinical and genetic description of 11 new patients. in JIMD Reports. JIMD Reports, vol. 44, Springer, pp. 85-92. https://doi.org/10.1007/8904_2018_128

TY - CHAP

T1 - DPAGT1 deficiency with encephalopathy (DPAGT1-CDG)

T2 - Clinical and genetic description of 11 new patients

AU - Ng, Bobby G.

AU - Underhill, Hunter R.

AU - Palm, Lars

AU - Bengtson, Per

AU - Rozet, Jean Michel

AU - Gerber, Sylvie

AU - Munnich, Arnold

AU - Zanlonghi, Xavier

AU - Stevens, Cathy A.

AU - Kircher, Martin

AU - Nickerson, Deborah A.

AU - Buckingham, Kati J.

AU - Josephson, Kevin D.

AU - Shendure, Jay

AU - Bamshad, Michael J.

AU - Freeze, Hudson H.

AU - Eklund, Erik A.

PY - 2019

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N2 - Pathogenic mutations in DPAGT1 cause a rare type of a congenital disorder of glycosylation termed DPAGT1-CDG or, alternatively, a milder version with only myasthenia known as DPAGT1-CMS. Fourteen disease-causing mutations in 28 patients from 10 families have previously been reported to cause the systemic form, DPAGT1-CDG. We here report on another 11 patients from 8 families and add 10 new mutations. Most patients have a very severe disease course, where common findings are pronounced muscular hypotonia, intractable epilepsy, global developmental delay/intellectual disability, and early death. We also present data on three affected females that are young adults and have a somewhat milder, stable disease. Our findings expand both the molecular and clinical knowledge of previously published data but also widen the phenotypic spectrum of DPAGT1-CDG.

AB - Pathogenic mutations in DPAGT1 cause a rare type of a congenital disorder of glycosylation termed DPAGT1-CDG or, alternatively, a milder version with only myasthenia known as DPAGT1-CMS. Fourteen disease-causing mutations in 28 patients from 10 families have previously been reported to cause the systemic form, DPAGT1-CDG. We here report on another 11 patients from 8 families and add 10 new mutations. Most patients have a very severe disease course, where common findings are pronounced muscular hypotonia, intractable epilepsy, global developmental delay/intellectual disability, and early death. We also present data on three affected females that are young adults and have a somewhat milder, stable disease. Our findings expand both the molecular and clinical knowledge of previously published data but also widen the phenotypic spectrum of DPAGT1-CDG.

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BT - JIMD Reports

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DPAGT1 deficiency with encephalopathy (DPAGT1-CDG): Clinical and genetic description of 11 new patients

Abstract

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